LU86866A1 - TETRAHYDRONAPHTHALINE DERIVATIVES - Google Patents

Description

*,., 8 6 8 6 6 v vvv .., r; t, ciïi, Ti VU; : Demande de Brevet convention ...................... .....................-_________________________ ii, ï. Requete

Le. société ...... dite: ....... F.HOFFMANN-LA ROCHE & CO. Aktiengesellschaft ^ .124-184 Grenze chers feras se j, CE-40 02 BASEL f Suisse, représentée car. Monsieur.Jacques ...... de Muyser, agissant en qualité de mandataire ................................. ........................................ .......... .... ................ "............................. ............ .............................. {t et sir rai 1900 guajtre- vingt sept. 4 c heures, au Ministère de l’Économie et des Classes Moyennes. à Luxembourg- 1, c r'r-erri requête pour î obtention d'un brevet dlnvemion concernant * "Teurshyâror aphthalinaeriva re." ............ .5 2. la descrtptipn en langue. everywhere ............................................. de l'invention en trois · exemplaires: ï. ......... / ................. planches de dessin, en trois exemplaires: 4. ia qunu-n.-t des · tuxes versées au Bureau de l'Enregistrement à Luxembourg, le 6 ..... may 198 * 5 ia dt2cga;. ”.-. n dt pouvoir, datée de. .BasSi ......................................... it .2c mars 198 / dépare * n! _ tr. it. re>? .msabihic de cette décaratior ;. pue r * esi ipv appoint t est (sur: f 1.VTcVel KLAUS, '€ Air. Hellenrain, D-7858 WEIL / RHEIK, R.F.A.

1. Peter 1.0ELI3ER, 19 Hauptstrasse, CH-4132 MUTTENS, Suisse revendipue * nv pour la susdite demande de brevet k priorité d'une ides ·· demande: sî de 7: ............ ................... rr evêzs ............................. ..................... déposéeisi ers i8s ....... AP — sse ................ .................

le î9i ..... 13. may ...... 1986 ................... et ...... le ........ 26 février ..... ..1.98.7 ............................................. ...............................

sous Je \ 1f 00, .1938 / 86 ................. et Ne .......... 742/87 ........ ........................................

au noir de; !! .la déposante élit · élisent cAndcae pou * · kl; elle 1 et. si désigne, pour sors mandataire, a Luxembourg .35 boulevard ... Royal ............................. ..... ...> 12 s {>! »Ijte: nt s a. délivrance d un brevet d’inventio :; pour îobieî décrit et représenté dans les annexes susmenti *. nneet a * ec a; oun;. £ n-> cnt de cette délivrance à ........ ........... mois il E. Frocès-verba! ot Dtpôî -X aexànde dz rtie 'CnâUur e été «eposes au Mrrusve de" Eoork -rte e- des i ^ es Mc, enn = r é.e:': cc ée it rrop '* e; tr.i rCrâ. cl iva ^ -kour, en date du 6 mai 138 ~ * 'Fr; e V .-.>: rr ii' Fr · .- · r.; ee: des' _-- e ·, en:; t; .

1 ; . i.e. d_ pr.jc-né.é '.? ~ j -.' .. z ... -.1 "’ - · ./ 52,644

DEMANDING PRIORITY

the patent / gjgKK application. 5 In: Switzerland ': · .. 1 From: May 13, 19'86 (No. 1938/86) and! of February 26, 1987 (No. 742/87) ',

PATENT APPLICATION

in ! Luxembourg

Applicant: F. HOFFMANN-LA ROCHE & CO. Joint-stock company CH-4002 BASEL (Switzerland)

Re: "Tetrahydronaphthalene derivatives." .

\ * 9 »10 tetrahydronaphthalene derivatives 15 The present invention relates to new tetrahydronaphthalene derivatives of the general formula

HjC C "3 OH... 20 Cil-R1

ÇQ

ιι, σ rush, 3 3 25 wherein R1 o-, m- or p-hydroxyphenyl; 2,3-, 2,4-, 2.5-, 2,6-, 3,4- or 3,5-dihydroxyphenyl; or 2,3,4-, 2.3.5-, 2.4.5-, 2,4,6-, 3,4,5- or 2,3,6-trihydroxyphenyl.

30, The compounds of formula I can exist as trans or cis isomers or cis / trans isomer mixtures. In general, the trans compounds of the formula I are preferred. furthermore those with whom R o-, m- or 35 I, ·

Grn / 11.3.87 "- 2 - p-hydroxyphenyl, especially p-hydroxyphenyl.

The invention further relates to a process for the preparation of the compounds of formula I, pharmaceutical preparations based on the compounds of formula I.

Compounds of formula I in the treatment and prophylaxis of neoplasms and dermatoses and the use of the compounds of formula I in the manufacture of pharmaceutical preparations for the treatment and prophylaxis of such 10 diseases.

According to the invention, the compounds of the formula I can be prepared by using a compound of the general formula 15

HjCch3 ch3. 'i.

—C ’i = CH- R

20th

H, C CiL

3 3 · 11 1 where R is a radical R in which the 25 hydroxyl group (s) is protected, the protective group is split off.

All conventional hydroxy protecting groups can be considered as protecting groups. Examples of such protective groups 30 are ethers. in particular the 2-tetrahydropyranyl ether and silyl ether, such as the trimethylsily ether; furthermore alkyl ethers such as methyl ether; and esters. e.g. lower alkane carboxylic acid esters, such as acetates and carbonates. The protecting groups can be split off in a manner known per se by treatment with acids, bases or reducing agents. Ether protecting groups such as tetrahydropyranyl and tri-methylsilyl can be split off by treatment with acids such as -3-p-toluenesulfonic acid or Lewis acids such as BF 3 or BBr 3 3. Ester protecting groups such as acetates or carbonates are formed by treatment with bases, e.g. alcoholic or aqueous-alcoholic alkali hydroxide solution removed.

5

The compounds of general formula II can be obtained by reacting a compound of general formula 1 ° a 111 H, G CH, 15 J> with a compound of general formula 11

B - R IV

20, where either A is one of the radicals -CH (CH3) P + (Q) 3Y or -CH (CH) P (0) (OAlk) and B is formyl, 3 2 25 or Ά acetyl and B is one of the radicals -CH2P + (Q) represents 3Y or -CH P (O) (OAlk); 2 2 and Q aryl, especially phenyl, 30 Y the anion of an organic or inorganic acid, e.g. Br and Alk lower alkyl, e.g. Methyl and 11 R mean the same as above.

35 The implementation of the compounds of formulas III and IV

can be carried out according to the known methods of the Wittig or Horner - 4 - reaction.

With the Wittig reaction. i.e. when using a compound of formula III with A = -CH (CH3) P + (Q) 3Y or 5 of formula IV with B = -CH2P + (Q) 3Y ~, the

Components in the presence of an acid binding agent »e.g. in the presence of a strong base, e.g. Butyllithium, sodium hydride or the sodium salt of dimethyl sulfoxide, but primarily in the presence of an ethylene oxide such as 1,2-butylene oxide, optionally substituted by lower alkyl, optionally in a solvent, e.g. in an ether, such as diethyl ether or tetrahydrofuran, or in an aromatic hydrocarbon, such as benzene, in a temperature range between room temperature and the boiling point of the reaction mixture 15.

Of the inorganic acid anions Y, the chlorine and bromine ion or the hydrosulfate ion is preferred, of the organic acid anions the tosyloxy ion is preferred. The aryl radical Q 20 is preferably a phenyl radical or a substituted phenyl radical such as p-tolyl.

In the Horner reaction, i.e. when using a compound of formula III with A = -CH (CH) -P (0) (OAlk) or 25 of formula IV with B = -CH -P (O) (OAlk) the U tt

Components using a base and preferably in the presence of an inert organic solvent. e.g. with the help of sodium hydride in benzene, toluene, dimethylformamide, tetrahydrofuran, dioxane or 1,2-dimethoxyethane »or also with the help of a sodium alcoholate in an alkanol. e.g. Sodium methylate in methanol, condensed in a temperature range between 0 ° and the boiling point of the reaction mixture.

35 The alkoxy residues OAlk are primarily lower alkoxy residues with 1-6 carbon atoms. such as methoxy or ethoxy.

- 5 -

The compounds of formula I can be in trans or cis form. Most of them are produced in the trans form during manufacture. If necessary, cis fractions can be separated off in a manner known per se, if desired.

Unless their preparation is known or described below, the starting compounds of the formulas III and IV can be prepared analogously to known methods or the methods described below.

The compounds of formula I are therapeutically active. They have in particular anti-seborrheic, anti-keratinizing, anti-neoplastic and anti-allergic / anti-inflammatory activity, which can be shown with the test arrangements described below: A) The effect in the prevention of chemically induced 20 breast tumors can be determined according to the following procedure. Female Sprague-Dawley rats are kept under temperature and light controlled conditions, with free access to drinking water and feed. At the age of 50 days, each rat was given 15 mg of Dime-25 thylbenz (a) anthracene dissolved in arachis oil using a gastric tube. Treatment with the trial compounds begins 1 day after the carcinogen administration. The body weights of the test animals are recorded and the tumors palpated weekly and measured using a caliper.

D 2 30 The volumes are calculated using the formula ^ · d, where D is the larger and d the smaller diameter of the tumor ellipsoid. The trial is ended and evaluated after 11 weeks. In this experiment, in addition to the 30 confronters who only receive normal food 35, the following two groups of experimental animals are used: - 6 - 1. 33 rats, to which 30 mg / kg of test compound mixed with the feed are administered daily.

2. 36 rats to which S 90 mg / kg test compound are administered daily mixed with the feed.

B) The effect on tumors can also be determined on the transplantable chondrosarcoma of the rat using the following method. The solid tumor of a donor animal is finely divided and suspended in phosphate buffer / saline. 0.5 ml of the 30% tumor pulp is implanted subcutaneously in albino rats.

The transplanted rats are divided into experimental groups 15 of 8 animals each. The test compounds are suspended in arachis oil and administered orally by gavage five times a week for 24 days. The tumors are excised and weighed on day 24. The results are expressed in the quotient C / T, which is calculated as follows: 20 ^ mean tumor weight of the control mean tumor weight of the treated.

C) The antimetaplastic effect can also be determined in rats according to the following method. Female Holtzmann rats with a weight of approx. 100 g are ovariectomized after an acclimatization period of 8 days under thiogenal anesthesia and tested after a further 14 days. Two animals each are housed in a cage 30 with free access to feed containing approximately 2000 IU of analytically determined vitamin A. Before oral administration of the test compound, the animals are treated subcutaneously with 1 µg oestradiol benzoate and 250 µg testosterone propionate dissolved in 0.1 ml sesame oil for 6 consecutive days. Parenteral hormone application leads to the formation of a pure plaice stage in the vaginal area, i.e. a squamous metaplasia. 2 days after oral - 7 -

When the test substance is administered, the reaction result is again read on the vaginal epithelium. The area method according to Behrens and Kärber is used to calculate the mean effective doses.

5

The results of experiments AC with the compound of the formula I, p - [(E) -2- (5.6,7.8-TetEahydro-5,5.8,8-tetramethyl -2-naphthyl) propenyl] phenol are shown in Tables I- III listed.

10th

Table I

A) Prophylaxis of the chemically induced breast tumor 15 ____

Dose rats with average-average [mg / kg] tumors were number of tumors p.o. [%] of tumor volume per rat in mm3 [% of controls [% of controls] __ controls] __ 20 30 68 52.4 72.6 90 35 14.1 3.9

25 Table II

B) Effect on transplantable chondrosarcoma of the rat 30 dose quotient C / T of tumor weight of the untreated [mg / kg] treated control animals and the treated animals _ 1 35__ 3.8 - 8 -

Table III

C) Anti-metaplastic effect on the rat 5 ___

Compound relative activity all-trans retinoic acid 1 10 Compound I 0.91

The compounds of the formula I can be used for topical and systemic therapy of benign and malignant neoplasias, 15 for pre-malignant lesions, and also for systemic and topical prophylaxis of the affection mentioned.

They are also suitable for topical and systemic therapy for acne, psoriasis and other dermatoses associated with increased or pathologically altered cornification, as well as for inflammatory and allergic dermatological affections. The process products of the formula I can also be used to combat mucosal diseases with inflammatory or degenerative or metaplastic changes. The compounds of the formula I are notable in particular for low toxicity or better tolerance in comparison with known retinoids.

30th

The agents can be administered enterally, parenterally or topically in pharmaceutical use forms. For enteral application, e.g. Pills in the form of tablets. Capsules, dragees, syrups »suspensions, solutions 35 and suppositories. Agents in the form of infusion or injection solutions are suitable for parenteral administration.

- 9 -

The dosages in which the preparations are administered can vary depending on the type of application and route of use, and on the needs of the patients. In general, daily doses of about 5 0.1-50 mg / kg, preferably 1-15 mg / kg, are suitable for adults.

The preparations can be administered in one or more doses. A preferred dosage form are capsules with a content of approximately 5-200 mg of active ingredient.

10th

The preparations can contain inert or pharmacodynamically active additives. Tablets or granules e.g. can be a number of binders, fillers. Contain carrier substances or diluents. Liquid preparations can be in the form of a sterile, water-miscible solution, for example. In addition to the active ingredient, capsules can also contain a filler or thickener. Furthermore, taste-improving additives, as well as the substances usually used as preservatives, stabilizers, moisturizers and emulsifiers, and also salts for changing the osmotic pressure. Buffers and other additives may be present.

The above-mentioned carriers and diluents can be made of organic or inorganic substances. e.g. of water. Gelatin, milk sugar, starch, magnesium stearate, talc. Gum arabic, polyalkylene glycols and the like. The prerequisite is that all auxiliary substances used in the preparation of the preparations are non-toxic.

For topical use, the active ingredients are expediently in the form of ointments. Tinctures, creams, solutions. Lotions, sprays, suspensions and the like. 35 ointments and creams and solutions are preferred. These preparations intended for topical use can be prepared by admixing the process products as an active ingredient, non-toxic, inert, solid or liquid carriers which are customary in such preparations and are suitable for topical treatment.

5 Approximately 0.1-5%, preferably 0.3-2%, and approximately 0.1-5%, preferably approximately 0.3-2%, are expedient for topical use Suitable for ointments or creams.

10 An antioxidant, e.g. Tocopherol, N-methyl-y-tocopheramine and butylated hydroxyanisole or butylated hydroxytoluene can be added.

15 The following examples further illustrate the invention. The temperatures are given in degrees Celsius.

Example 1 20 82.3 g of p- [2- (5 »6.7,8-tetrahydro-5,5,8.8.-tetramethyl-2-naphthyl) propenyl] phenylacetate are suspended in 2 l of ethanol and a solution of 130 g Potassium hydroxide added in 600 ml of water. After stirring for 1 hour at room temperature, the mixture is acidified to 25 with dilute hydrochloric acid and extracted several times with ethyl acetate. The organic phase is washed four times with water, dried over sodium sulfate and evaporated. The crystalline residue can be recrystallized from hexane / ethyl acetate and gives 66 g of p - [(E) -2- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl-2-naph-30 thyl ) propenyl] phénol, melting point 140-142 ° C.

The starting material can be prepared as follows: 360 g [1- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl 35 -2-naphthyl) ethyl] -triphenylphosphonium bromide are suspended in 500 ml of tetrahydrofuran and at 0 ° C with 410 ml of n-butyllithium (1.6 molar in hexane). After stirring for 1 hour at 11 ° C., a solution of 94.5 g of 4-acetoxybenzaldehyde in 300 ml of tetrahydrofuran is added dropwise and the mixture is stirred for a further 2 hours at room temperature. The reaction mixture is then poured into 2 l of methanol / water (6: 4) 5 and extracted several times with hexane. The organic phase is washed three times with water and, after drying, evaporated with sodium sulfate. After filtration of the residue over silica gel (eluent hexane / ethyl acetate = 9: 1) and crystallization from hexane, 83 g of p- [2- (5,6,7,8-10-tetrahydro-5,5,8,8- tetramethyl -2-naphthyl) propenyl] phenyl acetate in colorless crystals, melting point 114-116 ° C.

Example 2 15 In analogy to Example 1, the m- [2- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl-2-naphthyl) propenyl] phenylacetate was hydrolysed by hydrolysis of m- [ (E) -2- (5.6.7,8-tetrahydro - 5,5,8,8-tetramethyl -2-naphthyl) propenyl] phenol, melting point 91-93 ° C.

20th

Example 3

In analogy to Example 1, the o - [(E) - was obtained by hydrolysis of o- [2- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl-2-naphthyl) -25 propenyljphenyl acetate. 2- (5,6.7.8-tetrahydro - 5,5,8,8-tetramethyl-2-naphthyl) propenyl] phenol, melting point 97-99 ° C.

The preparation of use forms of the compounds of formula I can be carried out in a conventional manner, e.g. using the examples below.

35 - 12 -

Example A

Hard gelatin capsules can be produced as follows: 5 components mq / capsule 1. spray-dried powder containing 75% compound I 200 2. sodium dioctyl sulfosuccinate 0.2 10 3. sodium carboxymethyl cellulose 4.8 4. microcrystalline cellulose 86.0 5. talc 8.0 6. Magnesium stearate l , o

Total 300 15

The spray-dried powder, which is based on the active ingredient, gelatin and microcrystalline cellulose and has an average particle size of the active ingredient of <1 μ (measured by means of autocorrelation spectroscopy), is moistened and kneaded with an aqueous solution of sodium carboxymethyl cellulose and sodium dioctylsulfosuccinate. The resulting mass is granulated, dried and sieved, and the granules obtained are mixed with microcrystalline cellulose, talc and magnesium stearate. The powder is filled into 25 size 0 capsules.

30 35 - 13 -

Example B

Tablets can be produced as follows: 5 ingredients mq / tablet 1. Compound I as finely ground powder 500 2. Milk sugar powder 100 100 3. Corn starch white 60 10 4. Povidone K30 8 5. Corn starch white 112 6. Talc 16 16. Magnesium stearate 4

Total 800 15

The finely ground substance is mixed with milk sugar and part of the corn starch. The mixture is moistened and kneaded with an aqueous solution of Povidone K30, and the resulting mass is granulated, dried and sieved. The granules are mixed with the remaining corn starch, talc and magnesium stearate and pressed into tablets of a suitable size.

Example C

25th

Soft gelatin capsules can be made as follows:

Components ma / capsule 30 1. Compound I 50 2. Triglyceride 450

A total of 500 10 g of compound I are dissolved in 90 g of medium-chain triglyceride with stirring, inert gassing and 35 light protection. This r-14 solution is processed as a capsule filling mass into soft gelatin capsules each containing 50 mg of active ingredient.

Example D 5

A lotion can be prepared as follows: Components 10 1. Compound I, finely ground 3.0 g 2. Carbopol 934 0.6 g 3. Sodium hydroxide q.s. ad pH 6 4. ethanol. 94% 50.0 g 5. demineralized water ad 100.0 g 15

The active ingredient is incorporated into the ethanol, 94% strength / water mixture under light protection. Carbopol 934 is stirred in until complete gelation and the pH is adjusted with sodium hydroxide.

20 25 30 35

Claims (5)

1. Compounds of the general formula H, C CII, CH,. · 5 X 1 1 \ ÇO) HC CH 10 J wherein R is o-, m- or p-hydroxyphenyl; 2,3-, 2,4-, 2.5-, 2.6-, 3,4- or 3,5-dihydroxyphenyl; or 2,3,4-, 2.3.5-, 2.4.5-, 2,4,6-, 3,4,5- or 2,3,6-trihydroxyphenyl. 15 2. Compounds according to claim 1, in which the olefinic double bond has a trans configuration. 3. p - [(E) -2- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl 20 -2-naphthyl) propenyl] phenol. 4. m - [(E) -2- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl -2-naphthyl) propenyl] phenol. 25 5. o - [(E) -2- (5,6,7,8-tetrahydro-5,5,8,8-tetramethyl -2-naphthyl) propenyl] phenol. 6. Compounds of the formula I 2 for use as medicinal products. 30th 7. Pharmaceutical preparations containing a compound of general formula I and a pharmaceutical carrier. 8. Use of a compound of general formula I 35 for the manufacture of pharmaceutical preparations for the treatment of neoplasias and dermatoses. »» - 16 - 9. A process for the preparation of compounds of general formula I from claim 1, characterized in that from a compound of general formula 5 H "C CH, CH,‘ J V 3, 5 JL I. / C 'CH- R 11 H, C CH, 5 j in which R ^ is a radical R ^ in which the hydroxy group (s) is or are protected, 15 the protective group is split off. *** 20 25 30 35